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Poster viewing and lunch

132P - Neoadjuvant zanidatamab for stage I node negative HER2 positive breast cancer (BC)

Date

12 May 2023

Session

Poster viewing and lunch

Presenters

Vicente Valero

Citation

Annals of Oncology (2023) 8 (1suppl_4): 101220-101220. 10.1016/esmoop/esmoop101220

Authors

V. Valero1, J. Mouabbi2, H. Alonzo2, A. Nwosu Ilheme3, R. Murthy2, X. Huang2, W. Qiao3, M. Patel3, P.R. Pohlmann2, G. Rauch3, C. Checka3, K. Hunt3, D. Tripathy4, F. Meric-Bernstam5, F. Symmans3

Author affiliations

  • 1 The M.D. Anderson Cancer Center, Houston/US
  • 2 The University of Texas M.D. Anderson Cancer Center, Houston/US
  • 3 The University of Texas M. D. Anderson Cancer Center, Houston/US
  • 4 The University of Texas M.D. Anderson Cancer Center, 77030 - Houston/US
  • 5 The University of Texas M. D. Anderson Cancer Center, 77030 - Houston/US

Resources

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Abstract 132P

Background

Outcome of patients (pts) w/ stage I node neg HER2+ treated w/ wkly paclitaxel x 12 doses and trastuzumab x 1yr is excellent (10yr RFS 96%). Therefore, trials to de-escalate chemo and use targeted therapy alone are underway. Zanidatamab is a novel, humanized, bispecific, immunoglobulin G isotype 1-like, monoclonal antibody directed against the juxtamembrane extracellular domain (ECD4) and the dimerization domain (ECD2) of HER2. This results in HER2 clustering that modulates signaling and leads to immune activation. Zanidatamab demonstrated antitumor activity in heavily pre-treated HER2+ metastatic BC with acceptable safety profile. We hypothesized that zanidatamab would be a safe and effective regimen for women w/ node neg stage I HER2+ BC.

Methods

Pts w/ 1-3cm, clinically node neg HER2+ BC were enrolled in this investigator-initiated clinical trial. Pts had HER2+ BC: HER2 3+ by IHC or IHC 2+ and ISH +. Pts received 2-wkly zani x6 prior to surgery. Pts with ER+ tumors also received neoadjuvant endocrine therapy: postmenopausal pts received letrozole 2.5mg daily, and premenopausal pts received tamoxifen 20mg daily or GNRH and letrozole 2.5mg on treating physician preference. The primary objective was to evaluate efficacy as determined by pathologic complete response (pCR). Secondary objectives included pathologic response by residual cancer burden (RCB), radiological response, and safety profile of zanidatamab.

Results

Eleven pts w/ HER2+ BC were enrolled. Median age was 61yrs old (range 30-72). Median tumor size was 2.2cm (range 1-3cm). Four pts were pre-menopausal. Six pts had tumors >2cm tumors. Three received tamoxifen and 3 letrozole. All pts completed 6 cycles of zanidatamab and had Sx. Four (36%) had pCR, 3 RCB1 (28%) and 4 RCB2 (36%). This met the success criterion of Simon’s design (>=3/17 pts with pCR) of targeting a 25% pCR rate against a 5% null rate. Treatment was tolerated well. There were no grade 3 or 4 toxicities. One pt had minor infusion-related reaction and grade 2 acne, and 1 grade 2 diarrhea.

Conclusions

Neoadjuvant zanidatamab for 3 months showed significant efficacy, (pCR/RCB-1 64%) w/ acceptable safety profile in pts w/ stage I node neg HER2+ BC. The trial is ongoing and has been modified to increase treatment duration to 5mths (10 cycles).

Legal entity responsible for the study

The authors.

Funding

Zymeworks Inc.

Disclosure

All authors have declared no conflicts of interest.

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